Substrate Filtering by the Active Site Crossover Loop in UCHL3 Revealed by Sortagging and Gain-of-function Mutations

机译：揭示了通过UCHL3中的活动站点交叉环路进行的基质过滤通过分类和功能获得变异

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摘要

Determining how deubiquitinating enzymes discriminate between ubiquitin-conjugated substrates is critical to understand their function. Through application of a novel protein cleavage and tagging technique, sortagging, we show that human UCHL3 and the Plasmodium falciparum homologue, members of the ubiquitin C-terminal hydrolase family, use a unique active site crossover loop to restrict access of bulky ubiquitin adducts to the active site. Although it provides connectivity for critical active site residues in UCHL3, physical integrity of the crossover loop is dispensable for catalysis. By enlarging the active site crossover loop, we have constructed gain-of-function mutants that can accept substrates that the parent enzyme cannot, including ubiquitin chains of various linkages.

机译：确定去泛素化酶如何区分结合泛素的底物对于理解其功能至关重要。通过应用一种新颖的蛋白质裂解和标记技术，进行分类，我们显示人UCHL3和恶性疟原虫的同源物（泛素C末端水解酶家族的成员）使用独特的活性位点交叉环来限制庞大的泛素加合物对活动站点。尽管它为UCHL3中的关键活性位点残基提供了连通性，但交叉环的物理完整性对于催化是必不可少的。通过扩大活性位点交叉环，我们构建了功能增益突变体，可以接受母体酶不能接受的底物，包括各种连接的泛素链。

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期刊名称 The Journal of Biological Chemistry
作者
Maximilian W. Popp; Katerina Artavanis-Tsakonas; Hidde L. Ploegh;
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作者单位

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年(卷),期 2009(284),6
年度 2009
页码 3593–3602
总页数 10
原文格式 PDF
正文语种
中图分类分子生物学;
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5. Functional Characterization of the Mammalian TRPV4 Channel: Yeast Screen Reveals Gain-of-Function Mutations. [D] . Doyle, Christina A. 2012

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6. Genetic Mutations in the S-loop of Human Glutathione Synthetase: Links Between Substrate Binding Active Site Structure and Allostery [O] . Brandall L. Ingle, Bisesh Shrestha, Margarita C. De Jesus, 2019

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7. Substrate Filtering by the Active Site Crossover Loop in UCHL3 Revealed by Sortagging and Gain-of-function Mutations*S⃞ [O] . Popp, Maximilian W., Artavanis-Tsakonas, Katerina, Ploegh, Hidde L. 2008

机译：揭示了通过UCHL3中的活动站点交叉环路进行的基质过滤通过分类和功能获得变异*S⃞

Substrate Filtering by the Active Site Crossover Loop in UCHL3 Revealed by Sortagging and Gain-of-function Mutations

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